APICA: Difference between revisions

{{SummarySheet}}

{{SubstanceBox/APICA}}

'''APICA''' (also known as '''SDB-001''', and '''2NE1''') is a novel synthetic [[psychoactive class::cannabinoid]] that produces modified [[cannabis|cannabis-like]] effects when [[routes of administration|administered]]. It has been shown to act as a potent [[agonist]] for the CB1 and CB2 [[cannabinoid]] [[receptors]].<ref name="Banister2015">{{cite journal | vauthors=((Banister, S. D.)), ((Stuart, J.)), ((Kevin, R. C.)), ((Edington, A.)), ((Longworth, M.)), ((Wilkinson, S. M.)), ((Beinat, C.)), ((Buchanan, A. S.)), ((Hibbs, D. E.)), ((Glass, M.)), ((Connor, M.)), ((McGregor, I. S.)), ((Kassiou, M.)) | journal=ACS chemical neuroscience | title=Effects of bioisosteric fluorine in synthetic cannabinoid designer drugs JWH-018, AM-2201, UR-144, XLR-11, PB-22, 5F-PB-22, APICA, and STS-135 | volume=6 | issue=8 | pages=1445–1458 | date=19 August 2015 | issn=1948-7193 | doi=10.1021/acschemneuro.5b00107}}</ref>

The name "2NE1" appears to be a reference to the South Korean all-girl K-Pop group,<ref>{{Citation | year=2022 | title=2NE1 | url=https://en.wikipedia.org/w/index.php?title=2NE1&oldid=1099525651}}</ref> a naming convention shared by the closely related chemical [[AKB48]]. In 2011, the two chemicals were first identified in Japan as a mixture in a product sold under the name "Fragrance Powder".<ref>{{cite journal | vauthors=((Uchiyama, N.)), ((Kawamura, M.)), ((Kikura-Hanajiri, R.)), ((Goda, Y.)) | journal=Forensic Toxicology | title=Identification of two new-type synthetic cannabinoids, N-(1-adamantyl)-1-pentyl-1H-indole-3-carboxamide (APICA) and N-(1-adamantyl)-1-pentyl-1H-indazole-3-carboxamide (APINACA), and detection of five synthetic cannabinoids, AM-1220, AM-2233, AM-1241, CB-13 (CRA-13), and AM-1248, as designer drugs in illegal products | volume=30 | issue=2 | pages=114–125 | date= July 2012 | url=http://link.springer.com/10.1007/s11419-012-0136-7 | issn=1860-8965 | doi=10.1007/s11419-012-0136-7}}</ref> APICA has since been available for sale as a grey-area [[research chemical]] through online vendors.

Synthetic cannabinoids are commonly [[smoked]] or [[vaporized]] to achieve a quick [[onset]] of effects and rapid [[offset]]. There is little information available about the use of APICA via other [[routes of administration]], although as with other synthetic cannabinoids it could be expected to be [[orally]] active when dissolved in a lipid, which may significantly extend its [[duration]]. It is insoluble in water, but dissolves in ethanol and lipids.{{citation needed}}

Unlike [[cannabis]], the chronic abuse of [[synthetic cannabinoids]] has been [[Synthetic_cannabinoid#Deaths|associated with multiple deaths]] and [[Synthetic cannabinoid#Harm potential|more dangerous side effects and toxicity]] in general. Therefore, it is strongly discouraged to take this substance for extended periods of time or in excessive doses. Thorough independent research and [[harm reduction practices]] are strongly advised if choosing to use this substance.

APICA, or N-(1-adamantyl)-1-pentyl-1H-indole-3-carboxamide, is a synthetic [[Chemical class::indole cannabinoid]]. Like many synthetic cannabinoids, it can be considered to be composed of four linked structures: core, bridge, head, and tail.<ref>{{Citation | title=Synthetic cannabinoids in Europe | url=https://www.emcdda.europa.eu/topics/pods/synthetic-cannabinoids}}</ref> In APICA, the core indole group is substituted at R₁ with a pentyl chain tail and at R₃ with a carboxamide bridge linking to an [[adamantanes|adamantyl]] head.  

APICA can be considered an analog of both [[AKB48]], which features an indazole in place of APICA's indole group, and [[STS-135]], in which the pentyl tail is further substituted with a terminal fluorine.  

APICA acts as a full agonist of the cannabinoid [[receptors]], with similar potency at both [[CB1]] and [[CB2]]. In vivo experiments measuring the response of rats to APICA and similar drugs found that APICA had a similar potency to Δ9-[[THC]] and around a third the potency of [[JWH-018]]. In comparison to these other cannabinoids, APICA appeared to elicit a longer duration of effect. Caution should be exercised in interpreting studies using animals, however, as effects may differ significantly in humans.<ref>{{cite journal | vauthors=((Banister, S. D.)), ((Wilkinson, S. M.)), ((Longworth, M.)), ((Stuart, J.)), ((Apetz, N.)), ((English, K.)), ((Brooker, L.)), ((Goebel, C.)), ((Hibbs, D. E.)), ((Glass, M.)), ((Connor, M.)), ((McGregor, I. S.)), ((Kassiou, M.)) | journal=ACS Chemical Neuroscience | title=The Synthesis and Pharmacological Evaluation of Adamantane-Derived Indoles: Cannabimimetic Drugs of Abuse | volume=4 | issue=7 | pages=1081–1092 | date=3 April 2013 | url=https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3715837/ | issn=1948-7193 | doi=10.1021/cn400035r}}</ref>  

Pharmacological studies have reported EC₅₀ values of 6.89 ± 0.11nM at CB1 and 7.54 ± 0.11nM at CB2.<ref name="Banister2015"></ref> It is likely that APICA shares many of the in vivo properties of [[Δ9-THC]]. However, the role of these interactions and how they result in the cannabinoid high has yet to be scientifically validated.

In vivo metabolic studies on APICA have shown that the drug is fully metabolized with none of the original compound detectable in urine. The major metabolites were mono- or dihydroxylated on the adamantyl ring system and monohydroxylated on the pentyl chain.<ref>{{cite journal | vauthors=((Sobolevsky, T.)), ((Prasolov, I.)), ((Rodchenkov, G.)) | journal=Drug Testing and Analysis | title=Study on the phase I metabolism of novel synthetic cannabinoids, APICA and its fluorinated analogue | volume=7 | issue=2 | pages=131–142 | date= February 2015 | issn=1942-7611 | doi=10.1002/dta.1756}}</ref>

{{effects/base

 

*'''[[Effect::Spontaneous physical sensations]]''' - The "body high" of APICA can be described as a sharp,  uncomfortable, all-encompassing, and electric tingling sensation that spreads over the body after initial ingestion. It maintains a consistent presence that quickly rises with the onset and hits its limit once the peak has been reached before immediately dissipating.

*'''[[Effect::Appetite enhancement]]''' - As with many other cannabinoids, APICA causes an increase in appetite<ref>{{cite book | veditors=((Mechoulam, R.)) | date= 1986 | title=Cannabinoids as therapeutic agents | publisher=CRC Press | isbn=9780849357725}}</ref>, known colloquially as "the munchies" in popular American and United Kingdom culture. Clinical studies and survey data have found that cannabis increases food enjoyment and interest in food.<ref name="HMW">{{Citation | year=2001 | title=How Marijuana Works | url=https://science.howstuffworks.com/marijuana.htm}}</ref> This is thought to be due to the way in which endocannabinoids in the hypothalamus activate cannabinoid receptors that are responsible for maintaining food intake.<ref name="HMW"></ref>

*'''[[Effect::Pain relief]]''' - Cannabinoids have been clinically demonstrated to provide pain relief via agonism of cannabinoid receptors CB₁ and CB₂, which extends to [[synthetic cannabinoid]] receptor agonists.<ref>{{cite journal | vauthors=((Martín-Sánchez, E.)), ((Furukawa, T. A.)), ((Taylor, J.)), ((Martin, J. L. R.)) | journal=Pain Medicine | title=Systematic Review and Meta-analysis of Cannabis Treatment for Chronic Pain | volume=10 | issue=8 | pages=1353–1368 | date= November 2009 | url=https://academic.oup.com/painmedicine/article-lookup/doi/10.1111/j.1526-4637.2009.00703.x | issn=1526-2375 | doi=10.1111/j.1526-4637.2009.00703.x}}</ref><ref>{{cite journal | vauthors=((Lynch, M. E.)), ((Campbell, F.)) | journal=British Journal of Clinical Pharmacology | title=Cannabinoids for treatment of chronic non-cancer pain; a systematic review of randomized trials: Cannabinoids for pain | volume=72 | issue=5 | pages=735–744 | date= November 2011 | url=https://onlinelibrary.wiley.com/doi/10.1111/j.1365-2125.2011.03970.x | issn=03065251 | doi=10.1111/j.1365-2125.2011.03970.x}}</ref>

*'''[[Effect::Perception of bodily heaviness]]''' or '''[[Perception of bodily lightness]]'''

*'''[[Effect::Dehydration]]'''

*'''[[Effect::Dry mouth]]''' - This is known colloquially as "cotton mouth" in popular American and United Kingdom culture.

|{{effects/cognitive|

*'''[[Effect::analysis suppression]]'''

*'''[[Effect::Psychosis]]''' - The prolonged usage of synthetic [[cannabinoids]] may increase one's disposition to psychosis,<ref name="Arseneault2004">{{cite journal | vauthors=((Arseneault, L.)), ((Cannon, M.)), ((Witton, J.)), ((Murray, R. M.)) | journal=The British Journal of Psychiatry | title=Causal association between cannabis and psychosis: examination of the evidence | volume=184 | issue=2 | pages=110–117 | date= February 2004 | url=https://www.cambridge.org/core/journals/the-british-journal-of-psychiatry/article/causal-association-between-cannabis-and-psychosis-examination-of-the-evidence/71BA37D16485F186CE7B6B785E5B69A4 | issn=0007-1250 | doi=10.1192/bjp.184.2.110}}</ref> particularly in vulnerable individuals with risk factors for psychotic illnesses (like a past or family history of schizophrenia).<ref name="Every-Palmer2011">{{cite journal | vauthors=((Every-Palmer, S.)) | journal=Drug and Alcohol Dependence | title=Synthetic cannabinoid JWH-018 and psychosis: An explorative study | volume=117 | issue=2–3 | pages=152–157 | date= September 2011 | url=https://linkinghub.elsevier.com/retrieve/pii/S0376871611000639 | issn=03768716 | doi=10.1016/j.drugalcdep.2011.01.012}}</ref><ref name="Schneir2011">{{cite journal | vauthors=((Schneir, A. B.)), ((Cullen, J.)), ((Ly, B. T.)) | journal=The Journal of Emergency Medicine | title=“Spice” Girls: Synthetic Cannabinoid Intoxication | volume=40 | issue=3 | pages=296–299 | date=1 March 2011 | url=https://www.sciencedirect.com/science/article/pii/S0736467910008802 | issn=0736-4679 | doi=10.1016/j.jemermed.2010.10.014}}</ref><ref name="Vearrier2010">{{cite journal | vauthors=((Vearrier, D.)), ((Osterhoudt, K. C.)) | journal=Pediatric Emergency Care | title=A Teenager With Agitation: Higher Than She Should Have Climbed | volume=26 | issue=6 | pages=462–465 | date= June 2010 | url=http://journals.lww.com/00006565-201006000-00016 | issn=0749-5161 | doi=10.1097/PEC.0b013e3181e4f416}}</ref>

{{effects/auditory|

{{#ask: [[Category:APICA]][[Category:Experience]]|format=ul|Columns=1}}

 

The toxicity and long-term health effects of recreational APICA use do not seem to have been studied in any scientific context and the [[Toxicity::exact toxic dosage is unknown]]. This is because APICA has very little history of human usage. Anecdotal evidence from people who have tried APICA within the community suggests that there do not seem to be any negative health effects attributed to simply trying this substance at low to moderate doses by itself and using it sparingly (but nothing can be completely guaranteed).

It is advised that those with severe pre-existing mental conditions should not ingest these substances due to the way they strongly amplify [[emotion enhancement|one's current state of mind and emotions]]. Also, as with [[THC]] and [[cannabis]], prolonged usage of synthetic [[cannabinoids]] including APICA may increase one's disposition to mental illness and psychosis,<ref name="Arseneault2004"/> particularly in vulnerable individuals with risk factors for psychotic illnesses (like a past or family history of schizophrenia).<ref name="Every-Palmer2011"/><ref name="Schneir2011"/><ref name="Vearrier2010"/>

As synthetic cannabinoids are active in the milligram range (with below 5mg being a common dose), it is important to [[Dosage|use proper precautions when dosing]] to avoid a negative experience and injury to oneself or others.

As with other synthetic cannabinoids, the chronic use of APICA can be considered [[Addiction potential::moderately addictive with a high potential for abuse]] and is capable of causing psychological dependence among certain users. When addiction has developed, cravings and [[withdrawal effects]] may occur if a person suddenly stops their usage.

Tolerance to many of the effects of APICA [[Time to full tolerance::develops with prolonged and repeated use]]. This results in users having to administer increasingly large doses to achieve the same effects. After that, it takes about [[Time to half tolerance::3 - 7 days]] for the tolerance to be reduced to half and [[Time to zero tolerance::1 - 2 weeks]] to be back at baseline (in the absence of further consumption). APICA presents cross-tolerance with [[Cross-tolerance::all [[cannabinoids]]]], meaning that after the consumption of APICA all [[Psychoactive class::cannabinoid]]s will have a reduced effect.

===Overdose===

 

==Legal status==

 

*'''United Kingdom''': APICA is a Class B controlled substance under the third-generation synthetic cannabinoids generic definition, which came into effect on December 14, 2016 and is illegal to possess, produce, supply, or import. <ref>{{Citation | title=The Misuse of Drugs Act 1971 (Amendment) Order 2016 | url=https://www.legislation.gov.uk/uksi/2016/1109/made}}</ref>

*[https://en.wikipedia.org/wiki/APICA_(synthetic_cannabinoid_drug) APICA (Wikipedia)]

*[https://isomerdesign.com/PiHKAL/explore.php?id=4705 APICA (Isomer Design)]